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Identification of the fatty acid activation site on human ClC-2

Cuppoletti, John ; Tewari, Kirti P. ; Chakrabarti, Jayati ; [et al.]

American Physiological Society ; 2017

In: American Journal of Physiology-Cell Physiology Vol. 312, No. 6 ( 2017-06-01), p. C707-C723

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In: American Journal of Physiology-Cell Physiology, American Physiological Society, Vol. 312, No. 6 ( 2017-06-01), p. C707-C723

Abstract: Fatty acids (including lubiprostone and cobiprostone) are human ClC-2 (hClC-2) Cl − channel activators. Molecular and cellular mechanisms underlying this activation were examined. Role of a four-amino acid PKA activation site, RGET 691 , of hClC-2 was investigated using wild-type (WT) and mutant (AGET, RGEA, and AGAA) hClC-2 expressed in 293EBNA cells as well as involvement of PKA, intracellular cAMP concentration ([cAMP] i ), EP 2 , or EP 4 receptor agonist activity. All fatty acids [lubiprostone, cobiprostone, eicosatetraynoic acid (ETYA), oleic acid, and elaidic acid] caused significant rightward shifts in concentration-dependent Cl − current activation (increasing EC 50 s) with mutant compared with WT hClC-2 channels, without changing time and voltage dependence, current-voltage rectification, or methadone inhibition of the channel. As with lubiprostone, cobiprostone activation of hClC-2 occurred with PKA inhibitor (myristoylated protein kinase inhibitor) present or when using double PKA activation site (RRAA 655 /RGEA 691 ) mutant. Cobiprostone did not activate human CFTR. Fatty acids did not increase [cAMP] i in hClC-2/293EBNA or T84 cells. Using T84 CFTR knockdown cells, cobiprostone increased hClC-2 Cl − currents without increasing [cAMP] i, while PGE 2 and forskolin-IBMX increased both. Fatty acids were not agonists of EP 2 or EP 4 receptors. L-161,982, a supposed EP 4 -selective inhibitor, had no effect on lubiprostone-activated hClC-2 Cl − currents but significantly decreased T84 cell barrier function measured by transepithelial resistance and fluorescent dextran transepithelial movement. The present findings show that RGET 691 of hClC-2 (possible binding site) plays an important functional role in fatty acid activation of hClC-2. PKA, [cAMP] i , and EP 2 or EP 4 receptors are not involved. These studies provide the molecular basis for fatty acid regulation of hClC-2.

Type of Medium: Online Resource

ISSN: 0363-6143 , 1522-1563

URL: Article

DOI: 10.1152/ajpcell.00267.2016

Language: English

Publisher: American Physiological Society

Publication Date: 2017

detail.hit.zdb_id: 1477334-X

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